Abstract

Survival outcomes for lung cancer, the leading cause of cancer-related mortality in the United States, remain poor. Improving lung cancer survival requires a multi-pronged approach, including smoking cessation and better elucidation of gene-environment interactions in risk, identification of new promising drug targets, as well as identification of potential prognostic and predictive markers that can help optimize treatment for patients. Our molecular epidemiology research group has investigated lung cancer risk and geneenvironment interactions in the first SPORE cycle,.and supported by R01 funding. Other proposed SPORE projects are directly addressing new potential targets for drug interventions. In SPORE Project 1, we will focus on identifying prognostic and predictive markers of survival in lung cancer. The ultimate goal of identifying such markers is to find ways to select the best treatment course for each patient. Recent studies by our group have demonstrated the importance of germline polymorphic variants as prognostic and predictive factors, but these studies have investigated only a few candidate polymorphisms relative to survival outcomes. In this SPORE renewal, we have adopted a high-density pathway approach to investigate more extensively and efficiently the role of entire pathways in survival outcomes. We selected pathways with biologic evidence for a role in tumor aggressiveness or treatment response. Although the eventual goal will be to evaluate germline DNA, serology, tumor-based tissue, and clinical factors in one cohesive model, at present we will focus on germline DNA to identify critical pathway markers. To achieve this goal, we will utilize a large'(n=1,000), mature NSCLC case series, early and late stages, with annotated DNA and clinical data to assess genetic variation in selected pathways as prognostic and predictive markers in NSCLC.
In Aim 1 (gene discovery), we will use the Illumina Bead Station GoldenGate assay system for genotyping of single nucleotide polymorphisms (SNPs), which allows large-scale genotyping for up to 1,536 customized SNPs, to systematically assess the effects of genetic variation in these pathways on survival outcomes in 60% of our large sample size (discovery phase). For polymorphisms that cannot be assayed with this system and for candidate genes to be used in a validation phase (Aim 2) on the whole population, we will utilize other in-house techniques in the Genomics Core, including Sequenom and ABI 7900 Taqman. Though our primary endpoint will be overall survival (OS), we will also assess disease-free survival (DPS) and progression-free survival (PFS), where appropriate.
Aims 3 -4 will include assessing the role of gender and other factors in the genetic predictors of survival among lung cancer patients, using both stratified and interaction analyses;and assessing additional candidate genes (e.g. EGFR) and pathways identified from companion basic and translational science studies (Projects 2-5) in lung cancer outcomes. The detailed . clinical annotation of our case series is a unique resource with which to investigate prognostic and predictive markers, as well as for gene-environment interactions, in lung cancer survival.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Specialized Center (P50)
Project #
5P50CA090578-07
Application #
7888224
Study Section
Special Emphasis Panel (ZCA1)
Project Start
Project End
Budget Start
2009-07-01
Budget End
2010-06-30
Support Year
7
Fiscal Year
2009
Total Cost
$287,614
Indirect Cost

  Institution

Name
Dana-Farber Cancer Institute
Department
Type
DUNS #
076580745
City
Boston
State
MA
Country
United States
Zip Code
02215

  Publications

VanderLaan, Paul A; Rangachari, Deepa; Majid, Adnan et al. (2018) Tumor biomarker testing in non-small-cell lung cancer: A decade of change. Lung Cancer 116:90-95
Xu, Yinghui; Liu, Hongliang; Liu, Shun et al. (2018) Genetic variant of IRAK2 in the toll-like receptor signaling pathway and survival of non-small cell lung cancer. Int J Cancer 143:2400-2408
Ji, Xuemei; Bossé, Yohan; Landi, Maria Teresa et al. (2018) Identification of susceptibility pathways for the role of chromosome 15q25.1 in modifying lung cancer risk. Nat Commun 9:3221
Guo, Yichen; Zhang, Ruyang; Shen, Sipeng et al. (2018) DNA Methylation of LRRC3B: A Biomarker for Survival of Early-Stage Non-Small Cell Lung Cancer Patients. Cancer Epidemiol Biomarkers Prev 27:1527-1535
Haines, Eric; Chen, Ting; Kommajosyula, Naveen et al. (2018) Palbociclib resistance confers dependence on an FGFR-MAP kinase-mTOR-driven pathway in KRAS-mutant non-small cell lung cancer. Oncotarget 9:31572-31589
Wang, Zhaoxi; Wei, Yongyue; Zhang, Ruyang et al. (2018) Multi-Omics Analysis Reveals a HIF Network and Hub Gene EPAS1 Associated with Lung Adenocarcinoma. EBioMedicine 32:93-101
Torous, Vanda F; Rangachari, Deepa; Gallant, Benjamin P et al. (2018) PD-L1 testing using the clone 22C3 pharmDx kit for selection of patients with non-small cell lung cancer to receive immune checkpoint inhibitor therapy: are cytology cell blocks a viable option? J Am Soc Cytopathol 7:133-141
Ferreiro-Iglesias, Aida; Lesseur, Corina; McKay, James et al. (2018) Fine mapping of MHC region in lung cancer highlights independent susceptibility loci by ethnicity. Nat Commun 9:3927
Zhou, Fei; Wang, Yanru; Liu, Hongliang et al. (2017) Susceptibility loci of CNOT6 in the general mRNA degradation pathway and lung cancer risk-A re-analysis of eight GWASs. Mol Carcinog 56:1227-1238
Rangachari, Deepa; Costa, Daniel B (2017) Moving the mountain in advanced non-small-cell lung cancer: evolving immunotherapies for a dire disease. Transl Cancer Res 6:S151-S157

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